Competition for Active TGFβ Cytokine Allows for Selective Retention of Antigen-Specific Tissue- Resident Memory T Cells in the Epidermal Niche

Toshiro Hirai; Yi Yang; Yukari Zenke; Haiyue Li; Virendra K. Chaudhri; Jacinto S. De La Cruz Diaz; Paul Yifan Zhou; Breanna Anh Thu Nguyen; Laurent Bartholin; Creg J. Workman; David W. Griggs; Dario A.A. Vignali; Harinder Singh; David Masopust; Daniel H. Kaplan

doi:10.1016/j.immuni.2020.10.022

Competition for Active TGFβ Cytokine Allows for Selective Retention of Antigen-Specific Tissue- Resident Memory T Cells in the Epidermal Niche

Toshiro Hirai, Yi Yang, Yukari Zenke, Haiyue Li, Virendra K. Chaudhri, Jacinto S. De La Cruz Diaz, Paul Yifan Zhou, Breanna Anh Thu Nguyen, Laurent Bartholin, Creg J. Workman, David W. Griggs, Dario A.A. Vignali, Harinder Singh, David Masopust, Daniel H. Kaplan

Microbiology

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56 Scopus citations

Abstract

Following antigen-driven expansion in lymph node, transforming growth factor-β (TGFβ) is required for differentiation of skin-recruited CD8⁺ T cell effectors into epidermal resident memory T (Trm) cells and their epidermal persistence. We found that the source of TGFβ -supporting Trm cells was autocrine. In addition, antigen-specific Trm cells that encountered cognate antigen in the skin, and bystander Trm cells that did not, both displayed long-term persistence in the epidermis under steady-state conditions. However, when the active-TGFβ was limited or when new T cell clones were recruited into the epidermis, antigen-specific Trm cells were more efficiently retained than bystander Trm cells. Genetically enforced TGFβR signaling allowed bystander Trm cells to persist in the epidermis as efficiently as antigen-specific Trm cells in both contexts. Thus, competition between T cells for active TGFβ represents an unappreciated selective pressure that promotes the accumulation and persistence of antigen-specific Trm cells in the epidermal niche.

Original language	English (US)
Pages (from-to)	84-98.e5
Journal	Immunity
Volume	54
Issue number	1
DOIs	https://doi.org/10.1016/j.immuni.2020.10.022
State	Published - Jan 12 2021

Bibliographical note

Publisher Copyright:
© 2020 Elsevier Inc.

Keywords

TGFβ
antigen
bystander Trm
competition
keratinocytes
niche
resident memory T cells
skin
αβ
αβ

UN SDGs

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Hirai, T., Yang, Y., Zenke, Y., Li, H., Chaudhri, V. K., De La Cruz Diaz, J. S., Zhou, P. Y., Nguyen, B. A. T., Bartholin, L., Workman, C. J., Griggs, D. W., Vignali, D. A. A., Singh, H., Masopust, D., & Kaplan, D. H. (2021). Competition for Active TGFβ Cytokine Allows for Selective Retention of Antigen-Specific Tissue- Resident Memory T Cells in the Epidermal Niche. Immunity, 54(1), 84-98.e5. https://doi.org/10.1016/j.immuni.2020.10.022

Hirai, T, Yang, Y, Zenke, Y, Li, H, Chaudhri, VK, De La Cruz Diaz, JS, Zhou, PY, Nguyen, BAT, Bartholin, L, Workman, CJ, Griggs, DW, Vignali, DAA, Singh, H, Masopust, D & Kaplan, DH 2021, 'Competition for Active TGFβ Cytokine Allows for Selective Retention of Antigen-Specific Tissue- Resident Memory T Cells in the Epidermal Niche', Immunity, vol. 54, no. 1, pp. 84-98.e5. https://doi.org/10.1016/j.immuni.2020.10.022

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abstract = "Following antigen-driven expansion in lymph node, transforming growth factor-β (TGFβ) is required for differentiation of skin-recruited CD8+ T cell effectors into epidermal resident memory T (Trm) cells and their epidermal persistence. We found that the source of TGFβ -supporting Trm cells was autocrine. In addition, antigen-specific Trm cells that encountered cognate antigen in the skin, and bystander Trm cells that did not, both displayed long-term persistence in the epidermis under steady-state conditions. However, when the active-TGFβ was limited or when new T cell clones were recruited into the epidermis, antigen-specific Trm cells were more efficiently retained than bystander Trm cells. Genetically enforced TGFβR signaling allowed bystander Trm cells to persist in the epidermis as efficiently as antigen-specific Trm cells in both contexts. Thus, competition between T cells for active TGFβ represents an unappreciated selective pressure that promotes the accumulation and persistence of antigen-specific Trm cells in the epidermal niche.",

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Competition for Active TGFβ Cytokine Allows for Selective Retention of Antigen-Specific Tissue- Resident Memory T Cells in the Epidermal Niche

Abstract

Bibliographical note

Keywords

UN SDGs

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